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富含亮氨酸胶质瘤失活-1自身免疫性脑炎的长期预后及炎症、神经元和胶质细胞损伤的相关生物标志物

Long-term outcomes in leucine-rich glioma inactivated-1 autoimmune encephalitis and associated biomarkers of inflammation and neuronal and glial injury.

作者信息

Borko Tyler L, Winters Phillip, Money Kelli M, Sillau Stefan, Eggmann Sadie, Selva Sean, Ritchie Alanna, Kammeyer Ryan, Owens Gregory P, Bennett Jeffrey L, Piquet Amanda L

机构信息

Midwestern University Arizona College of Osteopathic Medicine, Glendale, AZ, United States.

Department of Neurology, University of Colorado Anschutz Medical Campus, Aurora, CO, United States.

出版信息

Front Neurol. 2025 May 21;16:1583892. doi: 10.3389/fneur.2025.1583892. eCollection 2025.

Abstract

INTRODUCTION

Leucine-rich glioma inactivated 1 (LGI1) autoimmune encephalitis (AE) is characterized by seizures, as well as cognitive, memory, and behavioral disturbances. Blood-based biomarkers for inflammation and neuronal and glial injury have been evaluated as potential markers of disease severity and prognosis in AE.

METHODS

Patients diagnosed with LGI1 AE, confirmed by cell-based assay, were enrolled and followed prospectively to gather plasma samples for biomarker testing. Biomarkers of neuronal and glial injury included plasma neurofilament light chain (NfL), glial fibrillary acidic protein (GFAP), ubiquitin c-terminal hydrolase L1 (UCHL-1), tau, and cytokine markers of inflammation. Biomarker data were logarithmically transformed and analyzed using longitudinal regression with the ratio of means between LGI1 AE and non-inflammatory controls. Clinical data were collected and correlated with blood-based biomarkers to assess their relationship to disease severity and long-term outcomes.

RESULTS

Twenty-one LGI1 AE patients were enrolled from October 2018 to April 2024, and 16 migraine headache patients (56.3% male; average age: 58 years) served as non-inflammatory controls. One LGI1 AE patient in our cohort had a clinical relapse. Modified Rankin Score (mRS) and Montreal Cognitive Assessment (MoCA) improved over time. The mRS at symptom onset was 3.34 and dropped to 0.56 in a 5-year follow-up. Mean MoCA scores were 18.45 at the onset and increased to 29.40 in the 6-year follow-up. The model estimated geometric mean plasma NfL values at disease diagnosis to be 11.86 pg/mL; it was estimated to be 6.07 pg/mL when compared to non-inflammatory controls. The model also estimated the plasma GFAP values to be 77.70 pg/mL; it was estimated to be 36.26 pg/mL when compared to non-inflammatory controls. The trend of clinical improvement is paralleled with a slow decline in NfL and GFAP levels, returning to levels like our control population after 6 and 3 years, respectively. MoCA scores tended to recover more quickly in patients presenting with lower Nfl scores at symptom onset.

CONCLUSION

Improved clinical symptoms were correlated with improvements in initially high NfL and GFAP levels. In one patient with a clinical relapse, NfL and GFAP levels increased. NfL and GFAP may be useful biomarkers of disease progression in patients with LGI1 AE. However, additional studies are needed to better understand the effects of immunotherapy.

摘要

引言

富含亮氨酸的胶质瘤失活1(LGI1)自身免疫性脑炎(AE)的特征为癫痫发作以及认知、记忆和行为障碍。基于血液的炎症、神经元和神经胶质损伤生物标志物已被评估为AE疾病严重程度和预后的潜在标志物。

方法

纳入经细胞检测确诊为LGI1 AE的患者,并进行前瞻性随访,以采集血浆样本进行生物标志物检测。神经元和神经胶质损伤的生物标志物包括血浆神经丝轻链(NfL)、胶质纤维酸性蛋白(GFAP)、泛素C末端水解酶L1(UCHL-1)、tau以及炎症细胞因子标志物。对生物标志物数据进行对数转换,并使用纵向回归分析LGI1 AE与非炎症对照组之间的均值比。收集临床数据并与基于血液的生物标志物进行关联,以评估它们与疾病严重程度和长期预后的关系。

结果

2018年10月至2024年4月纳入了21例LGI1 AE患者,16例偏头痛患者(男性占56.3%;平均年龄:58岁)作为非炎症对照组。我们队列中的1例LGI1 AE患者出现临床复发。改良Rankin量表(mRS)和蒙特利尔认知评估量表(MoCA)随时间有所改善。症状发作时的mRS为3.34,在5年随访中降至0.56。MoCA平均得分在发作时为18.45,在6年随访中升至29.40。该模型估计疾病诊断时血浆NfL几何平均值得分为11.86 pg/mL;与非炎症对照组相比估计为6.07 pg/mL。该模型还估计血浆GFAP值为77.70 pg/mL;与非炎症对照组相比估计为36.26 pg/mL。临床改善趋势与NfL和GFAP水平的缓慢下降并行,分别在6年和3年后恢复到我们对照组人群的水平。症状发作时Nfl得分较低的患者MoCA得分往往恢复得更快。

结论

临床症状改善与最初较高的NfL和GFAP水平的改善相关。在1例临床复发患者中,NfL和GFAP水平升高。NfL和GFAP可能是LGI1 AE患者疾病进展的有用生物标志物。然而,需要更多研究来更好地了解免疫治疗的效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1929/12133544/def26ac48f5a/fneur-16-1583892-g001.jpg

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